Assessment of diffusion-weighted MRI in predicting response to neoadjuvant chemotherapy in breast cancer patients

To compare region of interest (ROI)-apparent diffusion coefficient (ADC) on diffusion-weighted imaging (DWI) measurements and Ki-67 proliferation index before and after neoadjuvant chemotherapy (NACT) for breast cancer. 55 women were enrolled in this prospective single-center study, with a final population of 47 women (49 cases of invasive breast cancer). ROI-ADC measurements were obtained on MRI before and after NACT and were compared to histological findings, including the Ki-67 index in the whole study population and in subgroups of “pathologic complete response” (pCR) and non-pCR. Nineteen percent of women experienced pCR. There was a significant inverse correlation between Ki-67 index and ROI-ADC before NACT (r = − 0.443, p = 0.001) and after NACT (r = − 0.614, p < 0.001). The mean Ki-67 index decreased from 45.8% before NACT to 18.0% after NACT (p < 0.001), whereas the mean ROI-ADC increased from 0.883 × 10–3 mm2/s before NACT to 1.533 × 10–3 mm2/s after NACT (p < 0.001). The model for the prediction of Ki67 index variations included patient age, hormonal receptor status, human epidermal growth factor receptor 2 status, Scarff-Bloom-Richardson grade 2, and ROI-ADC variations (p = 0.006). After NACT, a significant increase in breast cancer ROI-ADC on diffusion-weighted imaging was observed and a significant decrease in the Ki-67 index was predicted. Clinical trial registration number: clinicaltrial.gov NCT02798484, date: 14/06/2016.


Scientific Reports
| (2023) 13:614 | https://doi.org/10.1038/s41598-023-27787-x www.nature.com/scientificreports/ A recent study demonstrated that a significant increase in the breast tumor region of interest (ROI) ADC on DWI predicts complete pCR and radiologic responses after one cycle of NACT. The two-dimensional (2D) ROI-ADC measurement of a tumoral target component was accurate and superior to the three-dimensional (3D) whole-lesion-ADC histogram analysis obtained after segmentation of the whole tumor 15 .
The present study aimed to compare the 2D ROI-ADC measurement with the Ki-67 proliferation index before and after NACT to assess ADC changes as a predictive biomarker for changes in the Ki-67 index due to NACT in patients with invasive breast cancer.

Methods
Study design and patient selection. This was an analysis of a prospective single-center study conducted between January 2016 and December 2019 on women with invasive breast cancer 15 . This study was approved by the institution's ethics committee of University Hospital Brugmann (EC 2016/76 B077201628620/I/U) and was also registered at ClinicalTrials.gov (NCT02798484, 14/06/2016). All experiments were performed in accordance with relevant guidelines and regulations. All patients signed informed consent forms and were enrolled according to the following study criteria: Inclusion criteria: (1) female gender, age over 18 years; (2) core needle biopsy-proven invasive breast cancer; (3) indication for NACT; (4) performance status of 0-3 according to the ECOG/WHO/Zubrod score 25 ; and (5) evaluable pre-and post-NACT MRI examinations. Exclusion criteria: (i) contraindications to MRI examination; (ii) contraindications to NACT; and (iii) absence of surgery.
Fifty-five women with 57 invasive breast cancers were included in this study and underwent MRI before starting NACT. Five women were excluded because two of them did not undergo MRI after NACT and three of them did not undergo surgery; thus, the final study sample consisted of 47 women with 49 invasive breast cancers. All patients received the same NACT followed by surgery. NACT consisted of anthracycline-based therapy (4 cycles at intervals of 3-4 weeks), followed by taxane-based therapy (12 weekly cycles of paclitaxel). For patients with HER2-positive tumors (9 patients), trastuzumab was administrated concomitantly with the anthracycline-based regimen (Fig. 1). For each patient, MRI with DCE and DWI before and after the completion of NACT were obtained and analyzed. MRI acquisition. MRI examinations were performed on a 3-Tesla system (Philips Ingenia, Best, The Netherlands) using a dedicated breast coil (7-element SENSE) in the prone position. Gadoteric acid (0.2 mmol/kg; Dotarem 0.5 mmol/mL, Guerbet, Aulnay, France) was injected with a power injector (Medrad, Maastricht, The Netherlands). The following sequences were acquired in the axial plane: T2 SPAIR TSE, T1 TSE, diffusionweighted single-shot echo-planar imaging EPI (b = 0, 50, 400, and 800 s/mm 2 ), and dynamic eTHRIVE (3D T1-weighted gradient echo with fat saturation) with gadolinium administration (Supplementary Table S1). The images were sent to a picture archiving and communication system workstation for analysis 15 . Image analysis. One radiologist with 15 years of experience in the field of breast MRI interpreted the MRI findings according to the BI-RADS classification 26 . Tumors were identified on DCE subtraction images and localized on DWI before and after treatment. The longest diameter (LD) of the lesion was measured on the DCE subtracted images. The ROI-ADC measurement of the lesion was obtained on the ADC map. These data were acquired prospectively.
The quantitative assessment of DWI consists usually in drawing a region of interest (ROI) on the b value image and copying it onto the ADC map, or directly on the darkest part of the ADC map corresponding to the targeted restrictive area on the highest b value. The ADC values thus yield quantitative data expressed in the units 10 -3 mm 2 /s and provide unique quantitative information which can be used for tissue characterization and response assessment. The simplest and common method to quantify the ADC of a tissue is by using summary statistics with a mean ADC value of an ROI. In the present study, a small circular ROI was placed on the darkest part of the lesion on the ADC map focused on the targeted restrictive regions corresponding to the highest signal intensity on the highest b-value, avoiding T2-shine through regions due to necrosis. The size of the ROI was www.nature.com/scientificreports/ adapted to the size of the signal intensity observed at the highest b value. In the case of multiple targeted components, multiple ROIs (three to five) were used, and the lowest ROI-ADC was retained. In the absence of a targeted restrictive residual tumor, the ROI was placed in the same tissue region as that in the previous examination. The percentage of change in LD between the two MRI scans (pre-and post-NACT) was calculated as follows: (value before NACT − value after NACT) * 100/value before NACT. Radiologic response was evaluated using the response evaluation criteria in solid tumors (RECIST v1.1) based on the LD changes of the tumor on preand post-treatment MRI: complete response (CR) corresponds to the complete resolution of the original imaging finding, partial response (PR) corresponds to an LD decrease of > 30%, progressive disease refers to an LD increase of > 20% or the appearance of new lesions, and stable disease (SD) corresponds to LD interval changes that do not fulfill these three responses 27 . Histopathology. The histopathology of the percutaneous core needle biopsy before NACT and that of the surgical specimen after NACT were the reference standards 28,29 . Histological grading was performed according to the modified Scarff-Bloom-Richardson scoring and combined Nottingham classification. Hormone receptor (HR) positivity (estrogen receptor positivity or progesterone receptor positivity) and human epidermal growth factor receptor 2 (HER2) expression were determined from core needle biopsies using immunohistochemistry (IHC). The Ki-67 proliferation index was determined by IHC on the core needle biopsy and surgical specimen (with a Dako MIB-1 antibody). The Ki-67 proliferation index was appraised on 100 cells count on a "hotspot. " Tumors were classified based on the IHC results according to the following molecular subtypes: luminal A (ERpositive, Ki-67 < 20%, and HER2-negative), luminal B (ER-positive with either Ki-67 ≥ 20% or HER2-positive); HER2 enriched (ER-negative and HER2-positive), and triple negative (ER-negative, PR-negative, and HER2negative). The histology of the surgical specimen was scored according to the 8th edition of the TNM Classification of Malignant Tumors 30 . The pathologic complete response (pCR) reference standard was based on histological analysis of the surgical specimen according to the residual cancer burden (RCB) system 31 . Patients were categorized as having pCR or non-pCR based on the postsurgical histopathological examination findings. pCR was defined as the absence of a residual tumor in the breast and axilla (ypT0 and ypN0) independent of the presence of ductal carcinoma in situ. pCR was evaluated according to the RCB protocol, and data were entered into the RCB calculator of the MD Anderson Cancer Center website (https:// www. mande rson. org/ for-physi cians/ clini cal-tool-resou rces/ clini cal-calcu lators/ resid ual-cancer-burden. html), which automatically calculates the value as follows: RCB-0 = pCR, RCB-I = minimal residual disease, RCB-II = moderate residual disease, and RCB-III = extensive residual disease.
Statistical analysis. Data were analyzed using SPSS 26 statistical software (IBM SPSS Statistics) and R software version 4.1.2. Continuous variables were expressed as mean ± one standard deviation (SD), while categorical variables were expressed as number (frequency). We used the Shapiro-Wilk test to test the normal distribution of continuous variables. We then used the Mann-Whitney U or Kruskal-Wallis tests to compare the mean values of two or more than two groups, respectively. For comparison of categorical variables, we used either Fisher's exact test or Pearson's chi-square test, as indicated 32 . Wilcoxon matched-pair signed-rank test was used to compare the median values of the paired samples. Moreover, the Spearman correlation coefficient was calculated to examine the correlation between ROI-ADC and the Ki-67 index. A stepwise backward multiple linear regression that included possible confounding variables (such as, patient age, tumor LD, hormonal receptors status, HER2 status, immunohistochemistry results, SBR grade, and δADC) for the prediction of the δKi67 proliferation index after NACT and a multivariate logistic regression to predict pathologic response were done. ADC and Ki67 proliferation index variations (δ) were calculated as follow: (value before NACT − value after NACT)*100/value before NACT. Statistical significance was assumed when the p-value was < 0.05.

25-84 years) with 49 invasive breast cancer cases (Supplementary
Variations in Ki-67 index and ROI-ADC according to tumor characteristics. The Ki-67 index increased from 22.5% ± 24.7% in grade 1 tumors to 56.4% ± 25.7% in grade 3 tumors (p < 0.001), whereas ROI-ADC decreased from 1.720 × 10 -3 mm 2 /s ± 1.177 × 10 -3 mm 2 /s to 0.799 × 10 -3 mm 2 /s ± 0.186 × 10 -3 mm 2 /s (p = 0.026). There was a statistically significant difference in the Ki-67 index values according to the tumor molecular types: luminal A, luminal B, and non-luminal. Nonetheless, the mean ROI-ADC was higher in tumors with the luminal A type than in those with luminal B or non-luminal types, but the difference was not statistically significant (Table 1). Table 2 presents the tumor characteristics on histology and MRI before and after NACT. There was a statistically significant decrease of Ki-67 index and LD (p < 0.001), whereas ROI ADC significantly increased. Before NACT, there was a significant inverse correlation between Ki-67 index and ROI-ADC (r = − 0.443, p = 0.001) (Supplementary Fig. S1). A similar finding was noted after NACT (r = − 0.614, p < 0.001) (Supplementary Fig. S2)
There was an inverse correlation between Ki-67 index and ROI-ADC in the pCR and non-pCR groups after NACT. However, the variation in the pCR group was more pronounced (Fig. 2). The variations in LD on DCE, ROI ADC, and Ki-67 index before and after NACT decreased significantly from RCB class 0 to RCB class 3 ( Table 4, Fig. 3). ADC variation before and after NACT was predictive for pCR (Supplementary Table S4).
Variations in Ki-67 index and ROI-ADC according to radiologic response. According to the RECIST criteria, the decrease in LD on DCE and the Ki-67 index after NACT was significantly lower in lesions with SD than in lesions with PR or CR, similar to the increase in ROI-ADC (Table 4). No progressive disease was observed in the final study population.

Discussion
The present study compared the ROI-ADC measurement of a targeted tumor component and the Ki-67 proliferation index before and after NACT to assess the tumoral response of invasive breast cancer. The results of this study showed an inverse correlation between ROI-ADC and Ki-67 proliferation index after NAC in patients with breast cancer. This correlation remained valid after grouping the tumors according to their pCR or radiologic response. www.nature.com/scientificreports/ The Ki-67 proliferation index is a prognostic marker based on the molecular subtype of breast cancer and is increasingly used to assess and manage breast cancer 3,16 . In fact, changes in the Ki-67 proliferation index due to NACT can independently predict the prognosis of patients with breast cancer 17,18 21 . However, in our monocentric study population of invasive breast cancers selected for NACT, there was a correlation between a higher Ki-67 index and a lower ADC with regard to the histological grade of the tumor. Interestingly, the mean Ki-67 index was 46%, and the mean ROI-ADC value was 0.888 × 10 -3 mm 2 /s with a mean LD of 50 mm, which corresponds to very low-to-low ADC values considering the ADC ranges based on recent meta-analyses evaluating DWI in differentiating benign and malignant lesions 22,23 .
While some studies have reported correlations between ADC values and Ki-67 index in breast cancers, only very few data have been published on ADC values and Ki-67 index changes after NACT. Nevertheless, ADC and Ki-67 proliferation indices are both tumor markers. In the present study, the mean Ki-67 index before NACT was higher in patients who achieved pCR than in those who did not. There was no significant difference in the ROI-ADC values before NAC between pCR and non-pCR patients. Moreover, the results of the present study showed an inverse correlation between ROI-ADC and Ki-67 proliferation index after NAC in patients with breast cancer. This correlation remained valid after grouping the tumors according to their pCR or radiologic responses. Our results are consistent with the most comparable study published in 2019 by Luo et al., suggesting that comparison Table 3. Tumor characteristics of the study population according to pathologic complete response. HER2 human epidermal growth factor receptor 2, HR hormone receptor, pCR pathologic complete response, Ki-67 Ki-67 proliferation index, NACT neoadjuvant chemotherapy, ROI region of interest, ADC apparent diffusion coefficient, LD largest diameter, DCE-MRI dynamic contrast-enhanced magnetic resonance imaging, DWI diffusion-weighted imaging.  24 . The authors suggested that changes in ADC values might be used as a surrogate marker for changes in the Ki-67 index in the NACT response of patients with invasive breast cancer. Because the authors did not consider the radiologic response or the patients who achieved pCR, the comparison with our study was limited. This study had some limitations. First, only one radiologist performed ROI-ADC measurements. Second, only one pathologist assessed the Ki-67 proliferation index. However, the pathologist followed the recommendations of the international Ki-67 in breast cancer working published to minimize the variation in analytical practice and to standardize the methodology 3 . Our study has several strengths. All patients underwent two consecutive MRI examinations before and after the same NACT protocol. All MRI examinations were standardized and performed prospectively using the same 3-T magnet. The post-processing was standardized. This study demonstrated that ADC measurement is a powerful functional parameter that offers information on tumor cellularity and could provide reliable, fast, noninvasive, and inexpensive prediction of breast cancer response to NACT. DWI does not require contrast agent injection and lasts for only a few minutes. After NACT, a significant increase in breast    www.nature.com/scientificreports/ cancer ADC value on DWI was observed, which predicted a significant decrease in the Ki-67 index in patients with radiological response and in patients with pCR. Therefore, we recommend the systematic use of an ROI targeted at the lowest breast cancer ADC in patients before and after NACT. The results of this study demonstrate that an inverse correlation between ROI-ADC and Ki-67 proliferation index is observed after NACT in breast cancer patients with pCR and patients with radiologic response. This finding could validate the reliability of the ADC value as a routine biomarker in assessing breast cancer response to NACT. Further studies with larger cohorts of patients should be realized to confirm our results.

Data availability
The datasets generated during and/or analysed during the current study are available from the corresponding author on reasonable request.